Tyrosine 1101 of Tie2 Is the Major Site of Association of p85 and Is Required for Activation of Phosphatidylinositol 3-Kinase and Akt

Kontos, Christopher D.; Stauffer, Thomas P.; Yang, Wen-Pin; York, John D.; Huang, Liwen; Blanar, Michael A.; Meyer, Tobias; Peters, Kevin G.

doi:10.1128/mcb.18.7.4131

Cited by 205 publications

(176 citation statements)

References 68 publications

(91 reference statements)

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“…Enhanced EC survival in response to Ang1 has been shown to be dependent on activation of Akt by PI3-kinase (also known as PKB). 10,17,20,41 Akt promotes cell survival through its ability to phosphorylate Bad and procaspase-9. 42,43 In addition, a recent report has demonstrated that Ang1 increased EC survival by the induction of the apoptosis inhibitor, survivin, again through the PI3-kinase/Akt pathway.…”

Section: Tie2 Signal Transductionmentioning

confidence: 99%

“…15 In addition, the p85 subunit of phosphatidylinositol (PI) 3-kinase can interact specifically with the phosphorylated Tie2 through its SH2 domain. Although an initial report suggested that activated Tie2 does not associate with PI3-kinase, 16 subsequent studies have confirmed that activation of Tie2 leads to PI3-kinase activation, 17 the lipid products of which participate in the regulation of cell survival by activation of the serine/ threonine kinase, Akt. 18 Indeed, the PI3-kinase/Akt pathway has been shown to transduce the antiapoptotic effect of both vascular endothelial growth factor (VEGF) 19 and Ang1.…”

mentioning

confidence: 99%

“…18 Indeed, the PI3-kinase/Akt pathway has been shown to transduce the antiapoptotic effect of both vascular endothelial growth factor (VEGF) 19 and Ang1. 17,20 Recently, Akt has also been demonstrated to directly phosphorylate endothelial nitric oxide synthase (eNOS), leading to calcium/calmodulin-independent enzyme activation. 21,22 Endothelium-derived nitric oxide (NO) is a crucial mediator in the regulation of EC growth, survival, and angiogenesis.…”

mentioning

confidence: 99%

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Angiogenic Actions of Angiopoietin-1 Require Endothelium-Derived Nitric Oxide

Babaei

Teichert-Kuliszewska

Zhang

et al. 2003

The American Journal of Pathology

163

138

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Angiopoietin1 (Ang1) is a novel angiogenic factor with important actions on endothelial cell (EC) differentiation and vascular maturation. Ang1 has been shown to prevent EC apoptosis through activation of PI3-kinase/ Akt, a pathway that is also known to activate endothelium nitric oxide synthase (eNOS). Therefore, we hypothesized that the angiogenic effects of Ang1 would also be dependent on the PI3-kinase/Akt pathway, possibly mediated by increased eNOS activity and NO release. Treatment of human umbilical vein endothelial cells with recombinant Ang1* (300 ng/ml) for 15 minutes resulted in PI3-kinase-dependent Akt phosphorylation, comparable to that observed with vascular endothelial growth factor (VEGF) (50 ng/ml), and increased NO production in a PI3-kinase/Akt-dependent manner. Capillary-like tube formation induced by Ang1* in fibrin matrix at 24 hours (differentiation index, DI: 13.74 ؎ 0.76 versus control 1.71 ؎ 0.31) was abolished in the presence of the selective PI3-kinase inhibitor, LY294002 (50 mol/L) (DI: 0.31 ؎ 0.31, P < 0.01) or the NOS inhibitor, L-NAME (3 mmol/L) (DI: 4.10 ؎ 0.59, P < 0.01). In subcutaneous Matrigel implants in vivo, addition of recombinant Ang1* or wild-type Ang1 from conditioned media of COS-1 cells transfected with a pFLAG Ang1 expression vector, induced significant neovascularization to a degree similar to VEGF. Finally, angiogenesis in vivo in response to both Ang1 and VEGF was significantly reduced in eNOS-deficient compared with wild-type mice. In summary, our results demonstrate for the first time that endothelialderived NO is required for Ang1-induced angiogenesis, and that the PI3-kinase signaling mediates the activation of eNOS and NO release in response to

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Section: Tie2 Signal Transductionmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

See 1 more Smart Citation

Angiogenic Actions of Angiopoietin-1 Require Endothelium-Derived Nitric Oxide

Babaei

Teichert-Kuliszewska

Zhang

et al. 2003

The American Journal of Pathology

163

138

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“…Subcellular fractionation and immunofluorescence imaging of endogenous Akt suggest that it is strongly recruited to the PM in response to growth factor stimulation (Carvalho et al, 2000;Currie et al, 1999;. Furthermore, live-cell imaging of fluorescent Akt reporter constructs have revealed important insights such as isoform specificity, chemotaxis, phospholipid binding, conformational changes in Akt, nuclear activation and membrane diffusion rates, across a range of cell lines (Calleja et al, 2003;Gonzalez and McGraw, 2009;Kontos et al, 1998;Lasserre et al, 2008;Servant et al, 2000;Wang and Brattain, 2006). Numerous groups have assessed Akt recruitment to the PM in response to various stimuli in live cells by using GFP-tagged full-length Akt and Akt PH domain constructs.…”

Section: Introductionmentioning

confidence: 99%

An improved Akt reporter reveals intra- and inter-cellular heterogeneity and oscillations in signal transduction

Norris

Yang

Krycer

et al. 2017

Journal of Cell Science

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Akt is a key node in a range of signal transduction cascades and play a critical role in diseases such as cancer and diabetes. Fluorescentlytagged Akt reporters have been used to discern Akt localisation, yet it has not been clear how well these tools recapitulate the behaviour of endogenous Akt proteins. Here, we observed that fusion of eGFP to Akt2 impaired both its insulin-stimulated plasma membrane recruitment and its phosphorylation. Endogenous-like responses were restored by replacing eGFP with TagRFP-T. The improved response magnitude and sensitivity afforded by TagRFP-T-Akt2 over eGFP-Akt2 enabled monitoring of signalling outcomes in single cells at physiological doses of insulin with subcellular resolution and revealed two previously unreported features of Akt biology. In 3T3-L1 adipocytes, stimulation with insulin resulted in recruitment of Akt2 to the plasma membrane in a polarised fashion. Additionally, we observed oscillations in plasma membrane localised Akt2 in the presence of insulin with a consistent periodicity of 2 min. Our studies highlight the importance of fluorophore choice when generating reporter constructs and shed light on new Akt signalling responses that may encode complex signalling information.This article has an associated First Person interview with the first author of the paper.

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“…6 However, the role of SCF/KIT signaling in tumor angiogenesis is still unclear 7 to data, except for the role of SCF in the recruitment of bone marrow-derived progenitor cells, 6,[8][9][10] together with angiopoietin-1 and stromal derived factor 1 a.…”

mentioning

confidence: 99%

E7080, a novel inhibitor that targets multiple kinases, has potent antitumor activities against stem cell factor producing human small cell lung cancer H146, based on angiogenesis inhibition

Matsui¹,

Yamamoto²,

Funahashi³

et al. 2007

Intl Journal of Cancer

450

312

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E7080 is an orally active inhibitor of multiple receptor tyrosine kinases including VEGF, FGF and SCF receptors. In this study, we show the inhibitory activity of E7080 against SCF-induced angiogenesis in vitro and tumor growth of SCF-producing human small cell lung carcinoma H146 cells in vivo. E7080 inhibits SCF-driven tube formation of HUVEC, which express SCF receptor, KIT at the IC 50 value of 5.2 nM and it was almost identical for VEGFdriven one (IC 50 5 5.1 nM). To assess the role of SCF/KIT signaling in tumor angiogenesis, we evaluated the effect of imatinib, a selective KIT kinase inhibitor, on tumor growth of H146 cells in nude mice. Imatinib did not show the potent antitumor activity in vitro (IC 50 5 2,200 nM), because H146 cells did not express KIT. However, oral administration of imatinib at 160 mg/kg clearly slowed tumor growth of H146 cells in nude mice, accompanied by decreased microvessel density. Oral administration of E7080 inhibited tumor growth of H146 cells at doses of 30 and 100 mg/kg in a dose-dependent manner and caused tumor regression at 100 mg/kg. While anti-VEGF antibody also slowed tumor growth, it did not cause tumor regression. These results indicate that KIT signaling has a role in tumor angiogenesis of SCF-producing H146 cells, and E7080 causes regression of H146 tumors as a result of antiangiogenic activity mediated by inhibition of both KIT and VEGF receptor signaling. E7080 may provide therapeutic benefits in the treatment of SCF-producing tumors. ' 2007 Wiley-Liss, Inc.

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Tyrosine 1101 of Tie2 Is the Major Site of Association of p85 and Is Required for Activation of Phosphatidylinositol 3-Kinase and Akt

Cited by 205 publications

References 68 publications

Angiogenic Actions of Angiopoietin-1 Require Endothelium-Derived Nitric Oxide

Angiogenic Actions of Angiopoietin-1 Require Endothelium-Derived Nitric Oxide

An improved Akt reporter reveals intra- and inter-cellular heterogeneity and oscillations in signal transduction

E7080, a novel inhibitor that targets multiple kinases, has potent antitumor activities against stem cell factor producing human small cell lung cancer H146, based on angiogenesis inhibition

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